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Point mutations in an epigenetic factor lead to multiple types of bone tumors: role of H3.3 histone variant in bone development and disease

机译:表观遗传因子中的点突变导致多种类型的骨肿瘤:H3.3组蛋白变体在骨发育和疾病中的作用

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摘要

Coordinated post-translational modifications (PTMs) of nucleosomal histones emerge as a key mechanism of gene regulation by defining chromatin configuration. Patterns of histone modifications vary in different cells and constitute core elements of cell-specific epigenomes. Recently, in addition to canonical histone proteins produced during the S phase of cell cycle, several non-canonical histone variants have been identified and shown to express in a DNA replication-independent manner. These histone variants generate diversity in nucleosomal structures and add further complexity to mechanisms of epigenetic regulation. Cell-specific functions of histone variants remain to be determined. Several recent studies reported an association between some point mutations in the non-canonical histone H3.3 and particular types of brain and bone tumors. This suggests a possibility of differential physiological effects of histone variants in different cells and tissues, including bone. In this review, we outline the roles of histone variants and their PTMs in the epigenetic regulation of chromatin structure and discuss possible mechanisms of biological effects of the non-canonical histone mutations found in bone tumors on tumorigenesis in differentiating bone stem cells.
机译:通过定义染色质构型,核小体组蛋白的协调翻译后修饰(PTM)成为基因调控的关键机制。组蛋白修饰的模式在不同的细胞中变化,并构成细胞特异性表观基因组的核心要素。近来,除了在细胞周期的S期产生的典型组蛋白之外,还鉴定了几种非典型组蛋白变体,并表明它们以DNA复制非依赖性的方式表达。这些组蛋白变体在核小体结构中产生多样性,并进一步增加表观遗传调控机制的复杂性。组蛋白变体的细胞特异性功能仍有待确定。最近的几项研究报告了非规范组蛋白H3.3中的某些点突变与特定类型的脑和骨肿瘤之间的关联。这表明在不同的细胞和组织(包括骨骼)中,组蛋白变体具有不同的生理效应的可能性。在这篇综述中,我们概述了组蛋白变体及其PTM在染色质结构的表观遗传调控中的作用,并讨论了在骨肿瘤中发现的非典型组蛋白突变对分化的骨干细胞中肿瘤发生的生物学影响的可能机制。

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